Comparison of uridine and N1-methylpseudouridine mRNA platforms in development of an Andes virus vaccine

Author:

Kuzmin Ivan V.ORCID,Soto Acosta Ruben,Pruitt Layne,Wasdin Perry T.ORCID,Kedarinath Kritika,Hernandez Keziah R.,Gonzales Kristyn A.,Hill Kharighan,Weidner Nicole G.,Mire ChadORCID,Engdahl Taylor B.ORCID,Moon Woohyun J.,Popov Vsevolod,Crowe James E.ORCID,Georgiev Ivelin S.ORCID,Garcia-Blanco Mariano A.,Abbott Robert K.ORCID,Bukreyev AlexanderORCID

Abstract

AbstractThe rodent-borne Andes virus (ANDV) causes a severe disease in humans. We developed an ANDV mRNA vaccine based on the M segment of the viral genome, either with regular uridine (U-mRNA) or N1-methylpseudouridine (m1Ψ-mRNA). Female mice immunized by m1Ψ-mRNA developed slightly greater germinal center (GC) responses than U-mRNA-immunized mice. Single cell RNA and BCR sequencing of the GC B cells revealed similar levels of activation, except an additional cluster of cells exhibiting interferon response in animals vaccinated with U-mRNA but not m1Ψ-mRNA. Similar immunoglobulin class-switching and somatic hypermutations were observed in response to the vaccines. Female Syrian hamsters were immunized via a prime–boost regimen with two doses of each vaccine. The titers of glycoprotein-binding antibodies were greater for U-mRNA construct than for m1Ψ-mRNA construct; however, the titers of ANDV-neutralizing antibodies were similar. Vaccinated animals were challenged with a lethal dose of ANDV, along with a naïve control group. All control animals and two animals vaccinated with a lower dose of m1Ψ-mRNA succumbed to infection whereas other vaccinated animals survived without evidence of virus replication. The data demonstrate the development of a protective vaccine against ANDV and the lack of a substantial effect of m1Ψ modification on immunogenicity and protection in rodents.

Funder

University of Texas Medical Branch

Publisher

Springer Science and Business Media LLC

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